1. A NOOB’S GUIDE TO
ECG
drkupe.blogspot.com
drkupe
Irfan Ziad MD UCD
2. Electrocardiography-
is transthoracic interpretation of the
electrical activity of the heart over
time captured and externally recorded
by skin electrodes for diagnostic or
research purposes on human hearts.
What is ECG?
3. THE HISTORY OF ECG MACHINE
1903
A Dutch doctor and physiologist.
He invented the first
practical electrocardiogram and
received the Nobel Prize in
Medicine in 1924 for it
Willem Einthoven
NOW
Modern ECG machine
has evolved into compact electronic
systems that often include
computerized interpretation of the
electrocardiogram.
5. The graph paper recording produced by the machine is termed an
electrocardiogram,
It is usually called ECG or EKG
STANDARD
CALLIBRATION
Speed = 25mm/s
Amplitude = 0.1mV/mm
1mV 10mm high
1 large square 0.2s(200ms)
1 small square 0.04s (40ms) or
1 mV amplitude
6. 1. Place the patient in a supine or
semi-Fowler's position. If the
patient cannot tolerate being flat,
you can do the ECG in a more
upright position.
2. Instruct the patient to place their
arms down by their side and to
relax their shoulders.
3. Make sure the patient's legs are
uncrossed.
4. Remove any electrical devices, such
as cell phones, away from the
patient as they may interfere with
the machine.
5. If you're getting artifact in the limb
leads, try having the patient sit on
top of their hands.
6. Causes of artifact: patient
movement, loose/defective
electrodes/apparatus, improper
grounding.
HOW TO DO ELECTROCARDIOGRAPHY
An ECG with artifacts.
Patient, supine position
7. The limb electrodes
RA - On the right arm, avoiding thick muscle
LA – On the left arm this time.
RL - On the right leg, lateral calf muscle
LL- On the left leg this time.
The 6 chest electrodes
V1 - Fourth intercostal space, right sternal border.
V2 - Fourth intercostal space, left sternal border.
V3 - Midway between V2 and V4.
V4 - Fifth intercostal space, left midclavicular line.
V5 - Level with V4, left anterior axillary line.
V6 - Level with V4, left mid axillary line.
Electrodes
Usually consist of a conducting gel, embedded
in the middle of a self-adhesive pad onto
which cables clip. Ten electrodes are used for a
12-lead ECG.
Placement of electrodes
8. The ECG works mostly by detecting and
amplifying the tiny electrical changes on the
skin that are caused when the heart muscle
"depolarizes" during each heart beat.
How does an ECG work?
13. PEOPLE USUALLY REFER THE
ELECTRODES CABLES AS
DUDE, THAT’S
CONFUSING!
LEADS
should be correctly
defined as the tracing
of the voltage
difference between
the electrodes and is
what is actually
produced by the ECG
recorder.
LEADS
15. III
II
LEADS I, II, III
THEY ARE FORMED BY VOLTAGE TRACINGS BETWEEN
THE LIMB ELECTRODES (RA, LA, RL AND LL). THESE
ARE THE ONLY BIPOLAR LEADS. ALL TOGETHER THEY
ARE CALLED THE LIMB LEADS OR
THE EINTHOVEN’S TRIANGLE
RA LA
RL LL
I
16. LEADS aVR, aVL, aVF
THEY ARE ALSO DERIVED FROM THE LIMB ELECTRODES, THEY
MEASURE THE ELECTRIC POTENTIAL AT ONE POINT WITH
RESPECT TO A NULL POINT. THEY ARE THE AUGMENTED LIMB
LEADS
RA LA
RL LL
aVR
aVF
aVL
17. LEADS
V1,V2,V3,V4,V5,V6
THEY ARE PLACED DIRECTLY ON THE CHEST. BECAUSE
OF THEIR CLOSE PROXIMITY OF THE HEART, THEY DO
NOT REQUIRE AUGMENTATION. THEY ARE CALLED THE
PRECORDIAL LEADS
RA LA
RL LL
V1
V2
V3
V4
V5
V6
18. These leads help to determine heart’s electrical axis. The
limb leads and the augmented limb leads form the frontal
plane. The precordial leads form the horizontal plane.
19. Leads Anatomical representation of the heart
V1, V2, V3, V4 Anterior
I, aVL, V5, V6 left lateral
II, III, aVF inferior
aVR, V1 Right atrium
The Different Views Reflect The Angles At Which LEADS "LOOK" At
The Heart And The Direction Of The Heart's Electrical Depolarization.
21. THE NORMAL SIZE
<3 small square
< 2 large square
< 2 small square
<3-5 small square
22. If a wavefront of
depolarization
travels towards the
positive electrode, a
positive-going
deflection will result.
If the waveform
travels away from
the positive
electrode, a
negative going
deflection will be
seen.
Understanding
ECG Waveform
23. E CG
I NTE R P R E TA TI ON
The More You See, The More You Know
24. OBTAIN A N ECG, ACT CONFIDENT, READ THE PT DETAILS
25. OBTAIN A N ECG, ACT CONFIDENT, READ THE PT DETAILS
Some ECG machines come with interpretation software. This one says
the patient is fine. DO NOT totally trust this software.
26. Rate
Rhythm
Cardiac Axis
P – wave
PR - interval
QRS Complex
ST Segment
QT interval (Include T and U wave)
Other ECG signs
The best way to interpret an ECG is to do it step-by-step
28. CALCULATING RATE
300
the number of BIG SQUARE between R-R interval
Rate =
As a general interpretation, look at lead II at the bottom part of the ECG strip. This
lead is the rhythm strip which shows the rhythm for the whole time the ECG is
recorded. Look at the number of square between one R-R interval. To calculate
rate, use any of the following formulas:
1500
the number of SMALL SQUARE between R-R interval
OR
Rate =
30. If you think that the rhythm is not regular, count the number of electrical beats in a
6-second strip and multiply that number by 10.(Note that some ECG strips have 3
seconds and 6 seconds marks) Example below:
CALCULATING RATE
1 2 3 4 5 6 7 8
= (Number of waves in 6-second strips) x 10
= 8 x 10
= 80 bpm
Rate
There are 8 waves in this 6-seconds strip.
31. You can also count the number of beats on any one row over the ten-second strip
(the whole lenght) and multiply by 6. Example:
CALCULATING RATE
= (Number of waves in 10-second strips) x 6
= 13 x 6
= 78 bpm
Rate
32. Interpretation bpm Causes
Normal 60-99 -
Bradycardia <60 hypothermia, increased vagal tone (due to vagal
stimulation or e.g. drugs), atheletes (fit people)
hypothyroidism, beta blockade, marked intracranial
hypertension, obstructive jaundice, and even in
uraemia, structural SA node disease, or ischaemia.
Tachycardia >100 Any cause of adrenergic stimulation (including
pain); thyrotoxicosis; hypovolaemia; vagolytic drugs
(e.g. atropine) anaemia, pregnancy; vasodilator
drugs, including many hypotensive agents; FEVER,
myocarditis
CALCULATING RATE
34. Look at p waves and their relationship to QRS complexes.
Lead II is commonly used
Regular or irregular?
If in doubt, use a paper strip to map out consecutive beats and see whether the rate
is the same further along the ECG.
Measure ventricular rhythm by measuring the R-R interval and atrial rhythm by
measuring P-P interval.
RHYTHM
35. RHYTHM
ECG rhythm characterized by a usual rate of anywhere between 60-99 bpm,
every P wave must be followed by a QRS and every QRS is preceded by P
wave. Normal duration of PR interval is 3-5 small squares. The P wave is
upright in leads I and II
Normal Sinus Rhythm
38. RHYTHM
In disease (e.g. sick sinus syndrome) the SA node can fail in its pacing
function. If failure is brief and recovery is prompt, the result is only a missed
beat (sinus pause). If recovery is delayed and no other focus assumes
pacing function, cardiac arrest follows.
Sinus pause
39. RHYTHM
Atrial Fibrillation
A-fib is the most common cardiac arrhythmia involving atria.
Rate= ~150bpm, irregularly irregular, baseline irregularity, no visible p waves,
QRS occur irregularly with its length usually < 0.12s
40. RHYTHM
Atrial Flutter
Atrial Rate=~300bpm, similar to A-fib, but have flutter waves, ECG baseline
adapts ‘saw-toothed’ appearance’. Occurs with atrioventricular block (fixed
degree), eg: 3 flutters to 1 QRS complex:
41. RHYTHM
Ventricular Fibrillation
A severely abnormal heart rhythm (arrhythmia) that can be life-threatening.
Emergency- requires Basic Life Support
Rate cannot be discerned, rhythm unorganized
42. RHYTHM
Ventricular tachycardia
fast heart rhythm, that originates in one of the ventricles- potentially life-
threatening arrhythmia because it may lead to ventricular fibrillation, asystole,
and sudden death.
Rate=100-250bpm
43. RHYTHM
Torsades de Pointes
literally meaning twisting of points, is a distinctive form of polymorphic
ventricular tachycardia characterized by a gradual change in the
amplitude and twisting of the QRS complexes around the isoelectric
line. Rate cannot be determined.
44. RHYTHM
Supraventricular Tachycardia
SVT is any tachycardic rhythm originating above the ventricular
tissue.Atrial and ventricular rate= 150-250bpm
Regular rhythm, p is usually not discernable.
*Types:
•Sinoatrial node reentrant tachycardia (SANRT)
•Ectopic (unifocal) atrial tachycardia (EAT)
•Multifocal atrial tachycardia (MAT)
•A-fib or A flutter with rapid ventricular response. Without rapid ventricular
response both usually not classified as SVT
•AV nodal reentrant tachycardia (AVNRT)
•Permanent (or persistent) junctional reciprocating tachycardia (PJRT)
•AV reentrant tachycardia (AVRT)
45. RHYTHM
Atrial Escape
a cardiac dysrhythmia occurring when sustained suppression of sinus
impulse formation causes other atrial foci to act as cardiac pacemakers.
Rate= 60-80bpm, p wave of atrial escape has abnormal axis and different
from the p wave in the sinus beat. However QRS complexes look exactly
the same.
46. RHYTHM
Junctional Escape
Depolarization initiated in the atrioventricular junction when one or more
impulses from the sinus node are ineffective or nonexistent. Rate: 40-60
bpm, Rhythm: Irregular in single junctional escape complex; regular in
junctional escape rhythm, P waves: Depends on the site of the ectopic
focus. They will be inverted, and may appear before or after the QRS
complex, or they may be absent, hidden by the QRS. QRS is usually
normal
48. RHYTHM
Atrial premature beat (APB)
Arises from an irritable focus in one of the atria. APB produces different
looking P wave, because depolarization vector is abnormal. QRS complex
has normal duration and same morphology .
49. RHYTHM
Junctional Premature Beat
Arises from an irritable focus at the AV junction. The P wave associated with
atrial depolarization in this instance is usually buried inside the QRS complex
and not visible. If p is visible, it is -ve in lead II and +ve in lead aVR and it it
may occur before or after QRS.
50. RHYTHM
Premature Ventricular Complexes (PVCs)
is a relatively common event where the heartbeat is initiated by the heart
ventricles(arrow) rather than by the sinoatrial node, Rate depends on
underlying rhythm and number of PVCs. Occasionally irregular rhythm,
no p-wave associated with PVCs. May produce bizarre looking T wave.
51. RHYTHM
Asystole
a state of no cardiac electrical activity, hence no contractions of the
myocardium and no cardiac output or blood flow.
Rate, rhythm, p and QRS are absent
52. RHYTHM
Pulseless Electrical Activity (PEA)
Not an actual rhythm. The absence of a palpable pulse and myocardial
muscle activity with the presence of organized muscle activity (excluding
VT and VF) on cardiac monitor. Pt is clinically dead.
53. RHYTHM
Artificial pacemaker
Sharp, thin spike. Rate depends on pacemaker, p wave
maybe absent or present
Ventricular paced rhythm shows wide ventricular pacemaker
spikes
56. CARDIAC AXIS
Electrical impulse that travels towards the electrode produces an upright (positive)
deflection (of the QRS complex) relative to the isoelectric baseline. One that travels
away produces negative deflection. And one that travels at a right angle to the lead,
produces a biphasic wave.
The cardiac axis refers to the general direction of the heart's depolarization wavefront
(or mean electrical vector) in the frontal plane. With a healthy conducting system the
cardiac axis is related to where the major muscle bulk of the heart lies.
57. CARDIAC AXIS
Axis Lead I Lead II Lead III
Normal Positive Positive Positive/Negative
Right axis
deviation
Negative Positive Positive
Left axis
deviation
Positive Negative Negative
To determine cardiac axis look at QRS complexes of lead , II, III.
Remember, positive(upgoing) QRS omplex means the impulse travels towards
the lead. Negative means moving away.
61. Cardiac Axis Causes
Left axis deviation Normal variation in pregnancy, obesity; Ascites,
abdominal distention, tumour; left anterior
hemiblock, left ventricular hypertrophy, Q Wolff-
Parkinson-White syndrome, Inferior MI
Right axis deviation normal finding in children and tall thin adults,
chronic lung disease(COPD), left posterior
hemiblock, Wolff-Parkinson-White syndrome,
anterolateral MI.
North West emphysema, hyperkalaemia. lead transposition,
artificial cardiac pacing, ventricular tachycardia
CARDIAC AXIS
63. Normal P- wave
3 small square wide, and 2.5 small square high.
Always positive in lead I and II in NSR
Always negative in lead aVR in NSR
Commonly biphasic in lead V1
P -WAVE
64. P -WAVE
P pulmonale
Tall peaked P wave. Generally due to enlarged
right atrium- commonly associated with congenital
heart disease, tricuspid valve disease, pulmonary
hypertension and diffuse lung disease.
Biphasic P wave
Its terminal negative deflection more than 40 ms
wide and more than 1 mm deep is an ECG sign of
left atrial enlargement.
P mitrale
Wide P wave, often bifid, may be due to mitral
stenosis or left atrial enlargement.
66. PR INTERVAL
NORMAL PR INTERVAL
PR-Interval 3-5 small square (120-200ms)
Long PR interval
may indicate heart
block
Short PR interval
may disease like
Wolf-Parkinson-
White
67. PR-INTERVAL
First degree heart block
P wave precedes QRS complex but P-R intervals prolong (>5 small
squares) and remain constant from beat to beat
68. Second degree heart block
1. Mobitz Type I or Wenckenbach
Runs in cycle, first P-R interval is often normal. With successive beat, P-R
interval lengthens until there will be a P wave with no following QRS complex.
The block is at AV node, often transient, maybe asymptomatic
PR-INTERVAL
69. Second degree heart block
2. Mobitz Type 2
P-R interval is constant, duration is normal/prolonged. Periodically, no
conduction between atria and ventricles- producing a p wave with no
associated QRS complex. (blocked p wave).
The block is most often below AV node, at bundle of His or BB,
May progress to third degree heart block
PR-INTERVAL
70. Third degree heart block (Complete heart block)
No relationship between P waves and QRS complexes
An accessory pacemaker in the lower chambers will typically activate
the ventricles- escape rhythm.
Atrial rate= 60-100bpm. Ventricular rate based on site of escape
pacemaker. Atrial and ventricular rhythm both are regular.
PR-INTERVAL
71. PR-INTERVAL
Wolff–Parkinson–White syndrome
Accessory pathway (Bundle of Kent)
allows early activation of the ventricle
(delta wave and short PR interval)
Wolf Parkinson White Syndrome
One beat from a rhythm strip in V2
demonstrating characteristic findings in
WPW syndrome. Note the characteristic
delta wave (above the blue bar), the short
PR interval (red bar) of 0.08 seconds, and
the long QRS complex (green) at 0.12
seconds
73. QRS complex< 3 small square (0.06 - 0.10 sec)
QRS COMPLEX
NORMAL QRS COMPLEX
Prolonged indicates hyperkalemia or
bundle branch block
Increased amplitude
indicated cardiac hypertrophy
S amplitude in V1 + R
amplitude in V5 < 3.5
Q wave amplitude less than
1/3 QRS amplitude(R+S) or
< 1 small square
74. QRS COMPLEX
Left Bundle Branch Block (LBBB)
indirect activation causes left ventricle contracts
later than the right ventricle.
Right bundle branch block (RBBB)
indirect activation causes right ventricle
contracts later than the left ventricle
QS or rS complex in V1 - W-shaped
RsR' wave in V6- M-shaped
Terminal R wave (rSR’) in V1 - M-shaped
Slurred S wave in V6 - W-shaped
Mnemonic: WILLIAM Mnemonic: MARROW
76. ST SEGMENT
NORMAL ST SEGMENT
ST segment < 2-3 small square (80 to 120 ms)
ST segment is isoelectric
and at the same level as
subsequent PR-interval
77. ST SEGMENT
Flat (isoelectric) ± Same level with subsequent PR
segment
Elevation or depression of ST segment by 1 mm or
more, measured at J point is abnormal.
J point is the point between QRS and ST segment
NORMAL
ST SEGMENT
THERE ARE 2 TYPES OF MI
ST-ELEVATION MI (STEMI) NON ST-ELEVATION MI (NSTEMI)
AND
WE DECIDE THIS BY LOOKING AT THE ST SEGMENT IN ALL LEADS
OK, WE GONNA TALK ABOUT
MYOCARDIAL INFARCTION (MI)
78. ST-SEGMENT
Look at ST changes, Q wave in all leads. Grouping
the leads into anatomical location, we have this:
Ischaemic change can be attributed to
different coronary arteries supplying the
area.
Location of
MI
Lead with
ST changes
Affected
coronary
artery
Anterior V1, V2, V3,
V4
LAD
Septum V1, V2 LAD
left lateral I, aVL, V5,
V6
Left
circumflex
inferior II, III, aVF RCA
Right atrium aVR, V1 RCA
*Posterior Posterior
chest leads
RCA
*Right
ventricle
Right sided
leads
RCA
*To help identify MI, right sided and
posterior leads can be applied
Localizing MI
I
II
III
aVR
aVL
aVF
V1
V2
V3
V4
V5
V6
(LAD)
(RCA)
79. Criteria:
ST elevation in > 2 chest leads > 2mm elevation
ST elevation in > 2 limb leads > 1mm elevation
Q wave > 0.04s (1 small square).
*Be careful of LBBB
The diagnosis of acute myocardial infarction should be
made circumspectively in the presence of pre-existing
LBBB. On the other hand, the appearance of new LBBB
should be regarded as sign of acute MI until proven
otherwise
DIAGNOSING MYOCARDIAL INFARCTION (STEMI)
Definition of a pathologic Q wave
Any Q-wave in leads V2–V3 ≥ 0.02 s or QS complex in leads V2 and V3
Q-wave ≥ 0.03 s and > 0.1 mV deep or QS complex in leads I, II, aVL, aVF, or V4–V6 in any two
leads of a contiguous lead grouping (I, aVL,V6; V4–V6; II, III, and aVF)
R-wave ≥ 0.04 s in V1–V2 and R/S ≥ 1 with a concordant positive T-wave in the absence of a
conduction defect.
A little bit troublesome to remember? I usually take pathological Q wave as >1 small square deep
Pathologic Q waves are a sign of previous myocardial infarction.
80. ST SEGMENT
ST-ELEVATION MI (STEMI)
0 HOUR
1-24H
Day 1-2
Days later
Weeks later
Pronounced T Wave initially
ST elevation (convex type)
Depressed R Wave, and Pronounced T Wave. Pathological Q waves
may appear within hours or may take greater than 24 hr.- indicating full-
thickness MI. Q wave is pathological if it is wider than 40 ms or deeper
than a third of the height of the entire QRS complex
Exaggeration of T Wave continues for 24h.
T Wave inverts as the ST elevation begins to resolve. Persistent ST
elevation is rare except in the presence of a ventricular aneurysm.
ECG returns to normal T wave, but retains pronounced
Q wave. An old infarct may look like this
83. NSTEMI is also known as subendocardial or non Q-wave MI.
In a pt with Acute Coronary Syndrome (ACS) in which the ECG does not show ST
elevation, NSTEMI (subendocardial MI) is suspected if
ST SEGMENT
NON ST-ELEVATION MI (NSTEMI)
•ST Depression (A)
•T wave inversion with or without ST depression (B)
•Q wave and ST elevation will never happen
To confirm a NSTEMI, do Troponin test:
•If positive - NSTEMI
•If negative – unstable angina pectoris
84. ST SEGMENT
NON ST-ELEVATION MI (NSTEMI)
N-STEMI: acute coronary syndrome (with troponin increase). Arrows
indicate ischemic ST segment changes. Without appropriate treatment
in many cases STEMI infarction will occur.
85. A ST depression is more suggestive of myocardial ischaemia than infarction
1mm ST-segment depression
Symmetrical, tall T wave
Long QT- interval
MYOCARDIAL ISCHEMIA
ST SEGMENT
87. ST SEGMENT
DIGOXIN
Down sloping ST segment depression
also known as the "reverse tick" or
"reverse check" sign in
supratherapeutic digoxin level.
88. ST SEGMENT
Now, moving to
LEFT VENTRICULAR
HYPERTROPHY
RIGHT VENTRICULAR
HYPERTROPHY
AND
So, we have to start looking at the S waves and R waves
89. ST SEGMENT
Left ventricular hypertrophy (LVH)
Example:
Sokolow & Lyon Criteria: S (V1) + R(V5 or V6) > 35mm
Cornell Criteria: S (V3) + R (aVL) > 28 mm (men) or > 20 mm (women)
Others: R (aVL) > 13mm
S (V1) + R(V5) = 15 + 25 = 40mm
S(V3) + R (aVL)= 15 + 14 =29mm
R(aVL) =14 mm LVH!
To determine LVH, use one of the following Criteria:
90. Tall R waves in V4 and V5 with down sloping ST segment depression and T
wave inversion are suggestive of left ventricular hypertrophy (LVH) with strain
pattern. LVH with strain pattern usually occurs in pressure overload of the left
ventricle as in systemic hypertension or aortic stenosis.
Let’s see another example of LVH
LVH strain pattern
ST SEGMENT
91. ST SEGMENT
Right ventricular hypertrophy (RVH)
Example:
Right axis deviation (QRS axis >100o
)
V1(R>S), V6 (S>R)
Right ventricular strain T wave inversion
So, it’s RVH!
92. LVH RVH
Hypertension (most common cause)
Aortic stenosis
Aortic regurgitation
Mitral regurgitation
Coarctation of the aorta
Hypertrophic cardiomyopathy
Pulmonary hypertension
Tetralogy of Fallot
Pulmonary valve stenosis
Ventricular septal defect (VSD)
High altitude
Cardiac fibrosis
COPD
Athletic heart syndrome
ST SEGMENT
Common Causes of LVH and RVH
94. QT interval decreases when heart rate increases.
A general guide to the upper limit of QT interval. For HR = 70 bpm, QT<0.40 sec.
•For every 10 bpm increase above 70 subtract 0.02s.
•For every 10 bpm decrease below 70 add 0.02 s
As a general guide the QT interval should be 0.35- 0.45 s,(<2 large square) and
should not be more than half of the interval between adjacent R waves (R-R
interval)
:
QT- INTERVAL
< 2 large square
95. To calculate the heart rate-corrected QT interval QTc. Bazett's formula is used
Calculation of QT interval
1.Use lead II. Use lead V5 alternatively if lead II cannot be read.
2.Draw a line through the baseline (preferably the PR segment)
3.Draw a tangent against the steepest part of the end of the T wave. If the T wave has
two positive deflections, the taller deflection should be chosen. If the T wave is
biphasic, the end of the taller deflection should be chosen.
4.The QT interval starts at the beginning of the QRS interval and ends where the
tangent and baseline cross.
5.If the QRS duration exceeds 120ms the amount surpassing ,120ms should be
deducted from the QT interval (i.e. QT=QT-(QRS width-120ms) )
96. If abnormally prolonged or shortened, there is a risk of developing ventricular
arrhythmias
The QT interval is prolonged in congenital long QT syndrome, but QT
prolongation can also occur as a consequence of
•Medication (anti-arrhythmics, tricyclic antidepressants, phenothiazedes)
•Electrolyte imbalances
•Ischemia.
QT prolongation is often treated with beta blockers.
QT = 0.04 x 10 small square= 0.4s
RR = 0.04 x 18 small square= 0.72s
18 small square
10 small square
97. T-WAVE
Normal T wave
Asymmetrical, the first half having more gradual slope
than the second half
>1/8 and < 2/3 of the amplitude of corresponding R wave
Amplitude rarely exceeds 10mm
Abnormal T waves are symmetrical, tall, peaked, biphasic,
or inverted.
LQT is a rare inborn heart condition in
which repolarization of the heart is delayed
following a heartbeat. Example: Jervell and
Lange-Nielsen Syndrome or Romano-Ward
Syndrome
LONG QT SYNDROME
98. U-WAVE
Prominent U waves are most often seen in hypokalemia, but may be present
in hypercalcemia, thyrotoxicosis, or exposure to digitalis,epinephrine, and Class 1A and
3 antiarrhythmics, as well as in congenital long QT syndrome, and in the setting of
intracranial hemorrhage.
An inverted U wave may represent myocardial ischemia or left ventricular volume overload
The U wave is a wave on an electrocardiogram that is not always seen. It is
typically small, and, by definition, follows the T wave. U waves are thought to
represent repolarization of the papillary muscles or Purkinje fibers
Normal U waves are small, round and symmetrical and positive in lead II. It is
the same direction as T wave in that lead.
100. Narrow and tall peaked T wave (A) is an early sign
PR interval becomes longer
P wave loses its amplitude and may disappear
QRS complex widens (B)
When hyperkalemia is very severe, the widened QRS complexes merge with their
corresponding T waves and the resultant ECG looks like a series of sine waves (C).
If untreated, the heart arrests in asystole
T wave becomes flattened together with appearance of a prominent U
wave.
The ST segment may become depressed and the T wave inverted.
these additional changes are not related to the degree of hypokalemia.
HYPERKALAEMIA
HYPOKALAEMIA
101. Usually, signs are not obvious
Hypercalcemia is associated with short QT interval (A) and
Hypocalcemia with long QT interval (B).
Interval shortening or lengthening is mainly in the ST segment.
HYPERCALCEMIA/HYPOCALCEMIA
102. PULMONARY EMBOLISM
Tachycardia and incomplete RBBB differentiated PE from no PE.
SIQIIITIII = deep S wave in lead I, pathological Q wave in lead III, and inverted
T wave in lead III.
The ECG is often abnormal in PE, but findings are not sensitive, not specific
Any cause of acute cor pulmonale can cause the S1Q3T3 finding on the ECG.